Abstract
We have recently demonstrated that several types of genomic rearrangements (i.e., telomere sister chromatid exchange (T-SCE), genomic-SCE, or end-to-end fusions) were more often detected in long-term cultured murine telomerase deficient embryonic stem (ES) cells than in freshly prepared murine splenocytes, even through they possessed similar frequencies of critically short telomeres. The high rate of genomic rearrangements in telomerase deficient ES cells, when compared to murine splenocytes, may reflect the cultured cells' gained ability to protect chromosome ends with eroded telomeres allowing them to escape "end crisis". However, the possibility that ES cells were more permissive to genomic rearrangements than other cell types or that differences in the microenvironment or genetic background of the animals might consequentially determine the rate of T-SCEs or other genomic rearrangements at critically short telomeres could not be ruled out.
| Original language | English |
|---|---|
| Pages (from-to) | 1320-1322 |
| Number of pages | 3 |
| Journal | Cell Cycle |
| Volume | 4 |
| Issue number | 10 |
| DOIs | |
| State | Published - Oct 2005 |
Funding
We sincerely thank Dr. Lea Harrington and Miss Natalie Erdmann for providing reagents and critical comments during this study and Dr. Susan Bailey for critical reading of the manuscript and generously supplying advice and protocols. We acknowledge the support of the office of Biological and Environmental Research, U.S. Department of Energy under Contract DE-AC056-960R22464 with UT-Battelle LLC.
Keywords
- Critically short telomeres
- Telomerase deficiency
- Telomere sister chromatid exchange